Functional polycystin-1 dosage governs autosomal dominant polycystic kidney disease severity
Katharina Hopp, Christopher J. Ward, Cynthia J. Hommerding, Samih H. Nasr, Han-Fang Tuan, Vladimir G. Gainullin, Sandro Rossetti, Vicente E. Torres, Peter C. Harris
Katharina Hopp, Christopher J. Ward, Cynthia J. Hommerding, Samih H. Nasr, Han-Fang Tuan, Vladimir G. Gainullin, Sandro Rossetti, Vicente E. Torres, Peter C. Harris
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Research Article

Functional polycystin-1 dosage governs autosomal dominant polycystic kidney disease severity

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is caused by mutations to PKD1 or PKD2, triggering progressive cystogenesis and typically leading to end-stage renal disease in midlife. The phenotypic spectrum, however, ranges from in utero onset to adequate renal function at old age. Recent patient data suggest that the disease is dosage dependent, where incompletely penetrant alleles influence disease severity. Here, we have developed a knockin mouse model matching a likely disease variant, PKD1 p.R3277C (RC), and have proved that its functionally hypomorphic nature modifies the ADPKD phenotype. While Pkd1+/null mice are normal, Pkd1RC/null mice have rapidly progressive disease, and Pkd1RC/RC animals develop gradual cystogenesis. These models effectively mimic the pathophysiological features of in utero–onset and typical ADPKD, respectively, correlating the level of functional Pkd1 product with disease severity, highlighting the dosage dependence of cystogenesis. Additionally, molecular analyses identified p.R3277C as a temperature-sensitive folding/trafficking mutant, and length defects in collecting duct primary cilia, the organelle central to PKD pathogenesis, were clearly detected for the first time to our knowledge in PKD1. Altogether, this study highlights the role that in trans variants at the disease locus can play in phenotypic modification of dominant diseases and provides a truly orthologous PKD1 model, optimal for therapeutic testing.

Authors

Katharina Hopp, Christopher J. Ward, Cynthia J. Hommerding, Samih H. Nasr, Han-Fang Tuan, Vladimir G. Gainullin, Sandro Rossetti, Vicente E. Torres, Peter C. Harris

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Figure 7

Cystogenesis of Pkd1RC/del2 mice is associated with an increase in proliferation.

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Cystogenesis of Pkd1RC/del2 mice is associated with an increase in proli...
(A) Representative images of kidney tissue from P18 Pkd1RC/del2 mice, indicating increased proliferation in noncystic and cystic CDs (DBA) compared with that in WT. Reports on associations between cyst expansion and proliferation are controversial, but analysis of the CD showed a clear increase in cell division (36, 37, 79). Scale bars: 20 μm. (B) Graph summarizing data of 100 nondilated CD cysts and 20 small (<50 cells [S]), 10 medium (50–200 cells [M]), and 5 large (>200 cells) CD cysts (Supplemental Table 3) (n = 3/group). Statistical values were obtained by the Student’s t test (*P < 0.05, **P < 0.01, ***P < 0.001); error bars indicate ± SD.